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龙脑和麝香酮对血脑屏障体外模型 MDCK 和 MDCK-MDR1 细胞中天麻苷转运的影响。

Influence of borneol and muscone on geniposide transport through MDCK and MDCK-MDR1 cells as blood-brain barrier in vitro model.

机构信息

School of Chinese Materia Medica, Beijing University of Chinese Medicine, No. 6, Zhonghuan South Road, Wangjing, Chaoyang District, Beijing 100102, China.

出版信息

Int J Pharm. 2013 Nov 1;456(1):73-9. doi: 10.1016/j.ijpharm.2013.08.017. Epub 2013 Aug 21.

Abstract

The objective of this study was (1) to characterize geniposide transport through MDCK and MDCK-MDR1 cell lines to confirm its transport mechanism and (2) to evaluate the effect of borneol and muscone as enhancers of geniposide transport in the BBB models so as to explore the enhancement mechanism. Transport studies of geniposide were performed in both directions, from apical to basolateral and from basolateral to apical sides. Drug concentrations were analyzed by HPLC. Geniposide showed relatively poor absorption in MDCK and MDCK-MDR1 cells, apparent permeability coefficients ranging from 0.323×10(-6) to 0.422×10(-6) cm/s. The in vitro experiments showed that geniposide transport in both directions was not concentration dependent and saturable, indicating purely passive diffusion. The efflux ratio of geniposide was less than 2 in the two cell models, which suggested that geniposide was not P-gp substrates. Geniposide transport in both directions significantly increased when co-administrated with increasing concentrations of borneol and muscone. Actin staining results indicated that borneol and muscone increased geniposide transport in the BBB models may attribute to disassembly effect on tight junction integrity.

摘要

本研究的目的是

(1) 通过 MDCK 和 MDCK-MDR1 细胞系来表征京尼平苷的转运,以确认其转运机制;(2) 评估龙脑和麝香酮作为 BBB 模型中京尼平苷转运增强剂的作用,以探讨其增强机制。采用 HPLC 分析药物浓度。京尼平苷在 MDCK 和 MDCK-MDR1 细胞中的吸收较差,表观渗透系数范围为 0.323×10(-6)至 0.422×10(-6)cm/s。体外实验表明,京尼平苷在两个方向的转运均无浓度依赖性和饱和性,表明为单纯的被动扩散。在两种细胞模型中,京尼平苷的外排比小于 2,提示京尼平苷不是 P-糖蛋白的底物。当与龙脑和麝香酮的浓度增加共同给药时,京尼平苷在两个方向的转运均显著增加。肌动蛋白染色结果表明,龙脑和麝香酮可能通过破坏紧密连接的完整性来增加 BBB 模型中京尼平苷的转运。

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